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Cytoplasmic Viral RNA-Dependent RNA Polymerase Disrupts the Intracellular Splicing Machinery by Entering the Nucleus and Interfering with Prp8

机译:细胞质病毒依赖RNA的RNA聚合酶通过进入细胞核并干扰Prp8破坏细胞内剪接机制。

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摘要

The primary role of cytoplasmic viral RNA-dependent RNA polymerase (RdRp) is viral genome replication in the cellular cytoplasm. However, picornaviral RdRp denoted 3D polymerase (3Dpol) also enters the host nucleus, where its function remains unclear. In this study, we describe a novel mechanism of viral attack in which 3Dpol enters the nucleus through the nuclear localization signal (NLS) and targets the pre-mRNA processing factor 8 (Prp8) to block pre-mRNA splicing and mRNA synthesis. The fingers domain of 3Dpol associates with the C-terminal region of Prp8, which contains the Jab1/MPN domain, and interferes in the second catalytic step, resulting in the accumulation of the lariat form of the splicing intermediate. Endogenous pre-mRNAs trapped by the Prp8-3Dpol complex in enterovirus-infected cells were identified and classed into groups associated with cell growth, proliferation, and differentiation. Our results suggest that picornaviral RdRp disrupts pre-mRNA splicing processes, that differs from viral protease shutting off cellular transcription and translation which contributes to the pathogenesis of viral infection.
机译:细胞质病毒依赖RNA的RNA聚合酶(RdRp)的主要作用是在细胞质中复制病毒基因组。然而,表示为3D聚合酶(3D pol )的微核病毒RdRp也进入宿主核,其功能尚不清楚。在这项研究中,我们描述了一种新型的病毒攻击机制,其中3D pol 通过核定位信号(NLS)进入细胞核,并靶向mRNA加工前因子8(Prp8)来阻断pre-mRNA加工。 mRNA剪接和mRNA合成。 3D pol 的指状结构域与包含Jab1 / MPN结构域的Prp8的C端区域相关联,并干扰第二个催化步骤,导致套索形式的剪接积累中间。鉴定了被肠道病毒感染的细胞中被Prp8-3D pol 复合物捕获的内源性前mRNA,并将其分类为与细胞生长,增殖和分化相关的组。我们的结果表明,picornaviral RdRp破坏了mRNA的剪接过程,这与病毒蛋白酶关闭细胞转录和翻译不同,后者有助于病毒感染的发病机理。

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